42 (47.1% vs 33%), respectively, for FaDu cells and 1.3 (58.0% vs 44.7%) and 1.2 (92.5% vs 76.9%), respectively, for A431 cells compared to double treatment of XRT with C225 ( Table 3). Moreover, in both cell lines,
double treatment with 48-hour C225 exposure was less effective than C225 alone, an observation that suggests the participation of an early acceleration of cell proliferation, a radiation-induced reaction already described in A431 cell line by Schmidt-Ullrich and co-workers [19]. Interestingly, this possible adaptive response was not observed after the triple treatment, perhaps counteracted by simvastatin SRT1720 nmr ( Table 3). Taken together, the in vitro results suggest that simvastatin could decrease cell proliferation in combination with XRT and C225, being its
effect potentiated in long-term drug exposures, and provide new insights about the triple combination. Because of preliminary in vitro findings indicating a possible activity of simvastatin as cell proliferation inhibitor in combination with C225 and XRT, this study was continued to investigate simvastatin role in xenografts. In tumors derived from FaDu and A431 cell lines, single SB431542 research buy treatment with simvastatin alone had no effect on tumor growth. On the contrary, treatment with C225 or XRT significantly reduced tumor growth compared to untreated tumors, XRT being the most effective treatment ( Figures 1A and 2A). FaDu tumors were more sensitive to XRT and C225 than A431 ones as was also seen in clonogenic assays ( Table 3). To focus on the main interest of this study, we started experiments irradiating FaDu tumors with 3 Gy per day for 10 days in combination with C225 in the presence or absence of simvastatin. Irrespectively of simvastatin, XRT plus C225 induced a transitory complete regression of tumors that lasted around
7 days (Figure 1B). After that, tumor growth rebounded but showed lower rates of regrowth when the animals received simvastatin. Mannose-binding protein-associated serine protease The time that the tumors took to achieve the size they had at the start of the treatment experienced a considerable delay when simvastatin was added to XRT + C225. The delay in mice that received simvastatin was 46 ± 5.8 days compared to 29 ± 3.2 days in the absence of simvastatin (a difference of 17 days; P value = .065). From the start of XRT, the time for the tumor volume to triple in size was 53.7 ± 4.4 days versus 42.8 ± 1.4 days depending on the presence of simvastatin or not, respectively (a difference of 11 days; P value = .086). In A431-tumors, to prevent a complete response, XRT dose was lowered to 2 Gy per day for 10 days. Contrary to the FaDu xenografts, A431 tumors did not achieve a complete disappearance, but similarly it was found that the mice treated with simvastatin showed A431 tumors with lower rates of regrowth (Figure 2B). Consistently with a simvastatin-induced enhancement in tumor growth inhibition, the growth delay after irradiation for the tumors treated with simvastatin was 14.4 ± 5.